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Genetically Engineered Mouse Models of Gliomas: Technological Developments for Translational Discoveries

机译:胶质瘤的基因工程小鼠模型:转化发现的技术发展。

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摘要

The most common brain tumours, gliomas, have significant morbidity. Detailed biological and genetic understanding of these tumours is needed in order to devise effective, rational therapies. In an era generating unprecedented quantities of genomic sequencing data from human cancers, complementary methods of deciphering the underlying functional cancer genes and mechanisms are becoming even more important. Genetically engineered mouse models of gliomas have provided a platform for investigating the molecular underpinning of this complex disease, and new tools for such models are emerging that are enabling us to answer the most important questions in the field. Here, I discuss improvements to genome engineering technologies that have led to more faithful mouse models resembling human gliomas, including new cre/LoxP transgenic lines that allow more accurate cell targeting of genetic recombination, Sleeping Beauty and piggyBac transposons for the integration of transgenes and genetic screens, and CRISPR-cas9 for generating genetic knockout and functional screens. Applications of these technologies are providing novel insights into the functional genetic drivers of gliomagenesis, how these genes cooperate with one another, and the potential cells-of-origin of gliomas, knowledge of which is critical to the development of targeted treatments for patients in the clinic.
机译:最常见的脑肿瘤神经胶质瘤有明显的发病率。为了设计有效,合理的疗法,需要对这些肿瘤有详细的生物学和遗传学理解。在一个从人类癌症中产生前所未有数量的基因组测序数据的时代,解密潜在功能性癌症基因和机制的互补方法变得越来越重要。基因工程改造的神经胶质瘤小鼠模型为研究这种复杂疾病的分子基础提供了一个平台,并且出现了这种模型的新工具,这些新工具使我们能够回答该领域最重要的问题。在这里,我将讨论基因组工程技术的改进,这些技术已导致产生了更忠实的类似于人类神经胶质瘤的小鼠模型,包括新的cre / LoxP转基因品系,可以更精确地靶向基因重组的细胞,Sleeping Beauty和piggyBac转座子可整合转基因和遗传筛选和CRISPR-cas9用于生成基因敲除和功能筛选。这些技术的应用为神经胶质瘤发生的功能性遗传驱动因素,这些基因如何相互协作以及神经胶质瘤的潜在起源细胞提供了新颖的见解,而对于神经胶质瘤患者的靶向治疗的发展至关重要诊所。

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